Bio
Born and raised in a large extended family from Indianapolis, Indiana, Kynon Jade Benjamin is proud to be the first doctor in his family. Dr. Benjamin earned his GED with the support of his family before moving on to Indiana University–Purdue University Indianapolis (IUPUI). At IUPUI, Dr. Benjamin completed his work study at a neuroscience research laboratory, which started his scientific research journey. In his predoctoral studies, Dr. Benjamin designed and implemented drug delivery and drug development assays as well as developed bioinformatic pipelines for differential expression analysis for Angelman syndrome - a neurodevelopmental disorder. In his subsequent postdoctoral fellowship at the Lieber Institute for Brain Development and Johns Hopkins University School of Medicine, he developed computational pipelines for large-scale transcriptional (bulk and single-cell), genetic, and functional associations analyses in postmortem brain and brain (cerebral and striatal) organoids.
The primary goal of Dr. Benjamin’s research is to improve therapeutics for under-research communities (i.e., personalized medicine) via investigating ancestry differences for neurological disorders in relevant tissues. To this end, he uses and develops computational tools to examine the role of ancestry in the brain. In addition to this, Dr. Benjamin has established collaborations to use computational tools to address hypthesize driven question with publically available single-cell and bulk tissues.
Throughout his research career, Dr. Benjamin’s experiences have reinforced the critical need for diversity and creating inclusive spaces. As such, he has worked to provide mentorship and representation as well as advocate for opportunities for other underrepresented minorities.
Education
| Institute / University | Location | Degree/Field | Completion Year |
|---|---|---|---|
| Lieber Institute for Brain Development | Baltimore, MD | Postdoctoral Fellow in Computational Genetics | Current |
| Johns Hopkins University School of Medicine | Baltimore, MD | Postdoctoral Fellow in Computational Genetics | Current |
| Texas A&M University | College Station, TX | Ph.D. in Genetics | August 2017 |
| Rensselaer Polytechnic Institute | Troy, NY | B.S. in Biomedical Engineering | May 2012 |
| Indiana University, Purdue University, Indianapolis | Indianapolis, IN | Biomedical Engineering (transferred) | May 2010 |
Research Interests
Neurological research in African Americans to reduce health disparities (K99)
Funding NIH Institute/Center | National Institute on Minority Health and Health Disparities |
Grant ID | K99MD0169640 |
MOSAIC Scientific Society | The Association of American Medical Colleges (AAMC) |
In neuroscience and genomics, individuals with recent African ancestry (AA) account for less than 5% of large-scale research cohorts for brain disorders but are 20% more likely to experience a major mental health crisis. Furthermore, divergent responses to antipsychotics between AA and European ancestry (EA) have been linked to genetic differences. Understanding these genetic and/or regulatory differences between AA and EA in the human brain, is essential to the development of effective neurotherapeutics and potentially could decrease health disparities for neurological disorders.
- Identify and characterize ancestry-related expression
differences in postmortem brain from AA and EA
individuals.
Rationale: Preliminary results revealed significant transcriptional changes across the four brain regions in neurotypical controls with admixed AA associated with genetic ancestry. Hypothesis: Genetic variations influence ancestry-related transcriptional changes via alternative isoform usage. 1) Differently expressed (DE) genomic features (genes, transcripts, exons, and junctions) associated with genetic ancestry will be identified and characterized within admixed AA. 2) eQTL analysis will be preformed to identify genetic variants interacting with genetic ancestry and expression; and 3) The contribution of these genetic variants on ancestry-related expression differences will be determined.
- Identify and characterize of ancestry-related epigenetic
differences in the brain
Rationale: Transgenerational stress has been shown to affect health outcomes. Due to past policies and practices, individuals of AA may be differentially exposed to extreme stresses across generations, which are identified as potential risk factors for common disorders. Hypothesis: Epigenetic differences drive ancestry-related expression differences in the brain. 1) Differentially methylated regions (DMRs) and genetic variation associated with DNAm between ancestries will be identified and characterized using BrainSeq Consortium publicly available expression, genetic, and DNA methylation for the caudate nucleus (n=400) and dorsolateral prefrontal cortex (n=378). 2) The contribution of these DMRs and DNAm on ancestry-related expression differences will be determined.
- Evaluate ancestry-related genetic and epigenetic
correlations with complex traits in the post-mortem
brain
Rationale: The integration of genomic information with complex traits has been used to improve our understanding of disease mechanism and prioritized potential therapeutic targets. Genetic differences have been linked to divergent responses to antipsychotics, suggesting genetic background is important to understanding individual disease susceptibility. Hypothesis: Epigenetic differences drive ancestry-specific complex trait associations in the brain. 1) Causal variants impacting complex trains with ancestry-related expression and DNAm will be identified and characterized. 2) Transfer learning will be applied to improve causal variant detection for AA.